AI Article Synopsis

  • Influenza A viruses (IAVs) disrupt cellular gene expression by affecting mRNA splicing in human lung cells, leading to increased exon inclusion and decreased intron retention.
  • More than half of the altered mRNAs in IAV-infected cells show splicing changes without significant shifts in overall abundance, indicating IAVs specifically manipulate this process.
  • The study also highlights that certain alternative splicing events are unique to IAV infection and suggests that IAVs may hijack specific cellular proteins, like RED, to enhance viral mRNA splicing at the expense of host mRNA processing.

Article Abstract

Influenza A viruses (IAVs) use diverse mechanisms to interfere with cellular gene expression. Although many RNA-seq studies have documented IAV-induced changes in host mRNA abundance, few were designed to allow an accurate quantification of changes in host mRNA splicing. Here, we show that IAV infection of human lung cells induces widespread alterations of cellular splicing, with an overall increase in exon inclusion and decrease in intron retention. Over half of the mRNAs that show differential splicing undergo no significant changes in abundance or in their 3' end termination site, suggesting that IAVs can specifically manipulate cellular splicing. Among a randomly selected subset of 21 IAV-sensitive alternative splicing events, most are specific to IAV infection as they are not observed upon infection with VSV, induction of interferon expression or induction of an osmotic stress. Finally, the analysis of splicing changes in RED-depleted cells reveals a limited but significant overlap with the splicing changes in IAV-infected cells. This observation suggests that hijacking of RED by IAVs to promote splicing of the abundant viral NS1 mRNAs could partially divert RED from its target mRNAs. All our RNA-seq datasets and analyses are made accessible for browsing through a user-friendly Shiny interface (http://virhostnet.prabi.fr:3838/shinyapps/flu-splicing or https://github.com/cbenoitp/flu-splicing).

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7680258PMC
http://dx.doi.org/10.1093/nargab/lqaa095DOI Listing

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